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酸敏感离子通道 1a 的失活动力学对 pH 值非常敏感。

Deactivation kinetics of acid-sensing ion channel 1a are strongly pH-sensitive.

机构信息

Center for Membrane Biology, Department of Biochemistry and Molecular Biology, University of Texas Health Science Center, Houston, TX 77030

Center for Membrane Biology, Department of Biochemistry and Molecular Biology, University of Texas Health Science Center, Houston, TX 77030.

出版信息

Proc Natl Acad Sci U S A. 2017 Mar 21;114(12):E2504-E2513. doi: 10.1073/pnas.1620508114. Epub 2017 Mar 6.

Abstract

Acid-sensing ion channels (ASICs) are trimeric cation-selective ion channels activated by protons in the physiological range. Recent reports have revealed that postsynaptically localized ASICs contribute to the excitatory postsynaptic current by responding to the transient acidification of the synaptic cleft that accompanies neurotransmission. In response to such brief acidic transients, both recombinant and native ASICs show extremely rapid deactivation in outside-out patches when jumping from a pH 5 stimulus to a single resting pH of 8. Given that the resting pH of the synaptic cleft is highly dynamic and depends on recent synaptic activity, we explored the kinetics of ASIC1a and 1a/2a heteromers to such brief pH transients over a wider [H] range to approximate neuronal conditions better. Surprisingly, the deactivation of ASICs was steeply dependent on the pH, spanning nearly three orders of magnitude from extremely fast (<1 ms) at pH 8 to very slow (>300 ms) at pH 7. This study provides an example of a ligand-gated ion channel whose deactivation is sensitive to agonist concentrations that do not directly activate the receptor. Kinetic simulations and further mutagenesis provide evidence that ASICs show such steeply agonist-dependent deactivation because of strong cooperativity in proton binding. This capacity to signal across such a large synaptically relevant bandwidth enhances the response to small-amplitude acidifications likely to occur at the cleft and may provide ASICs with the ability to shape activity in response to the recent history of the synapse.

摘要

酸敏离子通道(ASICs)是由质子在生理范围内激活的三聚体阳离子选择性离子通道。最近的报道表明,突触后定位的 ASICs 通过响应伴随神经传递的突触小间隙的短暂酸化,有助于兴奋性突触后电流。对于这种短暂的酸性瞬间,重组和天然的 ASICs 在从 pH 5 的刺激跳跃到单个静止 pH 8 的外部补丁中表现出极其快速的失活。鉴于突触小间隙的静息 pH 值高度动态且取决于最近的突触活动,我们探索了 ASIC1a 和 1a/2a 异源二聚体对这种更宽 [H] 范围内的短暂 pH 瞬间的动力学,以更好地模拟神经元条件。令人惊讶的是,ASICs 的失活对 pH 值非常敏感,跨越了近三个数量级,从 pH 8 时的极快(<1 ms)到 pH 7 时的非常慢(>300 ms)。这项研究提供了一个配体门控离子通道的例子,其失活对不直接激活受体的激动剂浓度敏感。动力学模拟和进一步的突变提供了证据,表明 ASICs 表现出如此陡峭的激动剂依赖性失活,是因为质子结合具有强协同性。这种在如此大的突触相关带宽内进行信号传递的能力增强了对小幅度酸化的反应,这些酸化可能发生在缝隙中,并可能使 ASICs 具有根据突触的最近历史来塑造活动的能力。

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